WO2011089401A1 - Crystalline forms of a purine derivative - Google Patents

Crystalline forms of a purine derivative Download PDF

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Publication number
WO2011089401A1
WO2011089401A1 PCT/GB2011/000087 GB2011000087W WO2011089401A1 WO 2011089401 A1 WO2011089401 A1 WO 2011089401A1 GB 2011000087 W GB2011000087 W GB 2011000087W WO 2011089401 A1 WO2011089401 A1 WO 2011089401A1
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Prior art keywords
crystalline
salt
crystalline form
compound
ray powder
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PCT/GB2011/000087
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English (en)
French (fr)
Inventor
Benjamin Mark Skead
Christopher Peter Worrall
Jonathan Charles Christian Atherton
Julian Scott Northen
Philippe Fernandes
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Cyclacel Limited
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
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Publication date
Priority to US13/574,488 priority Critical patent/US8889861B2/en
Priority to EP16186685.0A priority patent/EP3150602B1/en
Priority to SG2012050696A priority patent/SG182439A1/en
Priority to ES11701855.6T priority patent/ES2613716T3/es
Priority to EP11701855.6A priority patent/EP2526101B1/en
Priority to KR1020187014008A priority patent/KR101927083B1/ko
Application filed by Cyclacel Limited filed Critical Cyclacel Limited
Priority to PL16186685T priority patent/PL3150602T3/pl
Priority to KR1020127021718A priority patent/KR101860806B1/ko
Priority to CN201180015141.5A priority patent/CN102985423B/zh
Priority to JP2012549413A priority patent/JP5951506B2/ja
Publication of WO2011089401A1 publication Critical patent/WO2011089401A1/en
Priority to US14/524,686 priority patent/US9573951B2/en

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    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D473/00Heterocyclic compounds containing purine ring systems
    • C07D473/02Heterocyclic compounds containing purine ring systems with oxygen, sulphur, or nitrogen atoms directly attached in positions 2 and 6
    • C07D473/16Heterocyclic compounds containing purine ring systems with oxygen, sulphur, or nitrogen atoms directly attached in positions 2 and 6 two nitrogen atoms
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    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/495Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with two or more nitrogen atoms as the only ring heteroatoms, e.g. piperazine or tetrazines
    • A61K31/505Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim
    • A61K31/519Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim ortho- or peri-condensed with heterocyclic rings
    • A61K31/52Purines, e.g. adenine
    • AHUMAN NECESSITIES
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    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C303/00Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides
    • C07C303/32Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of salts of sulfonic acids
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    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C309/00Sulfonic acids; Halides, esters, or anhydrides thereof
    • C07C309/01Sulfonic acids
    • C07C309/02Sulfonic acids having sulfo groups bound to acyclic carbon atoms
    • C07C309/03Sulfonic acids having sulfo groups bound to acyclic carbon atoms of an acyclic saturated carbon skeleton
    • C07C309/04Sulfonic acids having sulfo groups bound to acyclic carbon atoms of an acyclic saturated carbon skeleton containing only one sulfo group
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    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C309/00Sulfonic acids; Halides, esters, or anhydrides thereof
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    • C07C309/28Sulfonic acids having sulfo groups bound to carbon atoms of six-membered aromatic rings of a carbon skeleton
    • C07C309/29Sulfonic acids having sulfo groups bound to carbon atoms of six-membered aromatic rings of a carbon skeleton of non-condensed six-membered aromatic rings
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    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C51/00Preparation of carboxylic acids or their salts, halides or anhydrides
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    • C07C59/00Compounds having carboxyl groups bound to acyclic carbon atoms and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups
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    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C59/00Compounds having carboxyl groups bound to acyclic carbon atoms and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups
    • C07C59/235Saturated compounds containing more than one carboxyl group
    • C07C59/245Saturated compounds containing more than one carboxyl group containing hydroxy or O-metal groups
    • C07C59/255Tartaric acid
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    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C59/00Compounds having carboxyl groups bound to acyclic carbon atoms and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups
    • C07C59/235Saturated compounds containing more than one carboxyl group
    • C07C59/245Saturated compounds containing more than one carboxyl group containing hydroxy or O-metal groups
    • C07C59/265Citric acid
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    • C07C65/00Compounds having carboxyl groups bound to carbon atoms of six—membered aromatic rings and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups
    • C07C65/01Compounds having carboxyl groups bound to carbon atoms of six—membered aromatic rings and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups containing hydroxy or O-metal groups
    • C07C65/03Compounds having carboxyl groups bound to carbon atoms of six—membered aromatic rings and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups containing hydroxy or O-metal groups monocyclic and having all hydroxy or O-metal groups bound to the ring
    • C07C65/05Compounds having carboxyl groups bound to carbon atoms of six—membered aromatic rings and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups containing hydroxy or O-metal groups monocyclic and having all hydroxy or O-metal groups bound to the ring o-Hydroxy carboxylic acids
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01FMEASURING VOLUME, VOLUME FLOW, MASS FLOW OR LIQUID LEVEL; METERING BY VOLUME
    • G01F1/00Measuring the volume flow or mass flow of fluid or fluent solid material wherein the fluid passes through a meter in a continuous flow
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    • G01F1/10Measuring the volume flow or mass flow of fluid or fluent solid material wherein the fluid passes through a meter in a continuous flow by using mechanical effects using rotating vanes with axial admission
    • G01F1/115Measuring the volume flow or mass flow of fluid or fluent solid material wherein the fluid passes through a meter in a continuous flow by using mechanical effects using rotating vanes with axial admission with magnetic or electromagnetic coupling to the indicating device
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01PMEASURING LINEAR OR ANGULAR SPEED, ACCELERATION, DECELERATION, OR SHOCK; INDICATING PRESENCE, ABSENCE, OR DIRECTION, OF MOVEMENT
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    • G01P3/42Devices characterised by the use of electric or magnetic means
    • G01P3/44Devices characterised by the use of electric or magnetic means for measuring angular speed
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    • G01P3/4802Devices characterised by the use of electric or magnetic means for measuring angular speed by measuring frequency of generated current or voltage by using electronic circuits in general
    • GPHYSICS
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Definitions

  • the present invention relates to crystalline forms of a purine derivative.
  • the invention also relates to a pharmaceutical composition containing said crystalline forms as the active ingredient, and use thereof in the prevention or treatment of disease.
  • the invention further relates to a process for preparing the crystalline forms.
  • compound (I) having the chemical name (2R,3S)-3-(6- ((4,6-dimethylpyridin-3-ylmethylamino)-9-isopropyl-9H-purin-2-ylamino)pentan-2-ol, exhibits potent CDK inhibitory activity and thus has potential therapeutic applications in the treatment of proliferative disorders, immune-mediated and inflammatory disorders, autoimmune and autoimmune-mediated disorders, kidney disorders, cardiovascular disorders, ophthalmic disorders, neurodegenerative disorders, psychiatric disorders, viral disorders, metabolic disorders and respiratory disorders.
  • compound (I) displays surprisingly high potency in cellular toxicity studies in a range of different cell lines.
  • the present invention seeks to provide compound (I) in crystalline form.
  • the invention seeks to provide crystalline forms that retain the desired pharmacological activity of the compound.
  • the present invention seeks to provide crystalline forms of compound (I) that exhibit one or more improved properties over the amorphous form.
  • a first aspect of the invention relates to a crystalline form of compound (I),
  • the crystalline forms of the invention typically demonstrate one or more improved properties over the amorphous form. Suitable properties include, for example, better storage stability, improved ease of handling (flowability, compressibility, stability), easier purification, and easier synthetic scale up
  • a second aspect of the invention relates to a pharmaceutical composition
  • a pharmaceutical composition comprising a crystalline form as described above as an active ingredient and a pharmaceutically acceptable diluent, excipient or carrier.
  • a third aspect of the invention relates to a crystalline form as described above for use in medicine.
  • a fourth aspect of the invention relates to a crystalline form as described above for use in the prevention or treatment of proliferative disorders, immune-mediated and inflammatory disorders, autoimmune and autoimmune-mediated disorders, kidney disorders, cardiovascular disorders, ophthalmic disorders, neurodegenerative disorders, psychiatric disorders, viral disorders, metabolic disorders and/or respiratory disorders.
  • a fifth aspect of the invention relates to use of a crystalline form as described above in the preparation of a medicament for the prevention or treatment of proliferative disorders, immune-mediated and inflammatory disorders, autoimmune and autoimmune-mediated disorders, kidney disorders, cardiovascular disorders, ophthalmic disorders, neurodegenerative disorders, psychiatric disorders, viral disorders, metabolic disorders and/or respiratory disorders.
  • a sixth aspect of the invention relates to a method for the prevention or treatment of proliferative disorders, immune-mediated and inflammatory disorders, autoimmune and autoimmune-mediated disorders, kidney disorders, cardiovascular disorders, ophthalmic disorders, neurodegenerative disorders, psychiatric disorders, viral disorders, metabolic disorders and/or respiratory disorders, said method comprising administering a pharmacologically effective amount of a crystalline form as described above to a subject in need thereof.
  • a seventh aspect of the invention relates to processes for preparing crystalline forms as described above.
  • the crystalline forms of the invention may be characterised by a range of different analytical techniques, including x-ray powder diffraction and differential scanning calorimetry. Further details of these techniques and equipment are set forth in the accompanying examples section.
  • solvate or “solvated form” refers to a crystal having one or more molecules of solvent associated therewith as an inherent part of the crystal structure.
  • the solvate or solvated form is the hydrate.
  • different plural crystalline forms (polymorphs) of the same compound can be produced by varying the crystallisation conditions used. These different crystalline forms have different three-dimensional structures and different physicochemical properties.
  • the existence of polymorphs is inherently unpredictable and theoretical calculations to predict polymorphs are extremely unreliable, with many more polymorphs predicted than can actually be isolated in practice.
  • the crystalline forms of the invention are at least 95 % pure (in terms of the purity of the crystal form), more preferably, at least 97 % pure, even more preferably, at least 98 or 99 % pure (for example, as analysed by HPLC). More preferably still, the crystalline forms of the invention are at least 99.5 % pure.
  • the present invention encompasses the crystalline form of the free base of compound (I) as well as crystalline forms of various pharmaceutically acceptable salts thereof.
  • the invention encompasses crystalline forms of the L-tartrate, citrate, benzenesulfonate, mesylate, maleate, L-malate, fumarate, gentisate, hydrochloride, hydrobromide and phosphate salts of compound (I).
  • the hydrochloride salt exhibited several forms with the observation of four XRPD patterns with deliquescence or form changes observed at elevated RH.
  • the hydrobromide salt appeared to exist in two forms, one hygroscopic and the other only observed by storage at elevated RH.
  • the mesylate salt exhibited deliquescence at both 25 ° C/97% RH and 40/0/75% RH.
  • the maleate salt proved to be hygroscopic above 40°C/70% RH.
  • L-malate exhibited two crystalline forms, one exhibiting deliquescence at 40'C/75% RH, the second proving to be non-hygroscopic.
  • the gentisate salt appeared to exist in two forms, one a partially crystalline form and the other a crystalline mono salt that could be an acetonitrile solvate.
  • the crystalline free base (Form A) was found to be a non solvated form of compound (I), which melts at 132°C, is non-hygroscopic and has an aqueous solubility in water of 0.33 mg/ml.
  • Forms B and C can dehydrate on heating and/or reducing the ambient humidity to give two further anhydrous forms respectively.
  • the dehydration step is reversible on cooling and/or increasing humidity.
  • Form C was discovered to be the most stable hydrate, exhibiting low hygroscopicity, complete dehydration below 100°C, melt of the respective anhydrous Form at 125°C, and high aqueous solubility (> 20 mg. ml "1 ).
  • the L-tartrate salt (Form D) was found to be a non-hydrated, non-solvated 1 :1 salt with respect to tartaric acid and compound (I).
  • Form E The L-tartrate salt (Form E) was found to be a non-hydrated, non-solvated 1 :1 salt with respect to tartaric acid and compound (I). It exhibits a melt at 178°C, has high aqueous solubility (43.9 mg. ml "1 ) and is only slightly hygroscopic. Of the two tartrate salts Form E is the most stable form with a higher melting point. Form E is also less hygroscopic.
  • the citrate salt (Form F) was found to be a non-hydrated, non-solvated 1 :1 salt with respect to citric acid and compound (I). It exhibits a melt at 145°C, followed by decomposition, high aqueous solubility (> 15 mg.ml "1 ) and is hygroscopic above only 70%RH.
  • the benzenesulfonate salt (Form G) was found to be a non-hydrated, non-solvated 1 :1 salt with respect to benzenesulfonic acid and compound (I). It exhibits a melt at 147°C, high aqueous solubility (> 20 mg. ml "1 ) and is highly hygroscopic above 75%RH.
  • the crystalline free base Form A and the L-tartrate salt Form E are especially preferred as they are non-hydrated, are not highly hygroscopic and exhibit reasonably high melting points.
  • the Form E L-tartrate is the most preferred as it has a high melting point has good aqueous solubility and is only slightly hygroscopic.
  • the fumarate (Form P) salt is also highly preferred for the same reasons.
  • the crystalline forms of the invention can be obtained from a supersaturated solution.
  • the supersaturated solution can be prepared through dissolution of compound (I) in an appropriate solvent, optional pH adjustment of said solution, concentration of said solution, cooling said solution, addition of a solvent in which compound (I) is slightly soluble to a solution of compound (I) in a solvent in which compound (I) is readily soluble.
  • a suspension of a crystal or amorphous solid of compound (I) in an appropriate solvent is converted into a slurry and then is stirred to transform into an alternate crystalline form. This is known as solvent-mediated transformation.
  • precipitation of the crystals takes place spontaneously in the reaction vessel or can be started or accelerated by addition of a crystalline seed, by mechanical stimulation such as through use of ultrasonic waves or by scratching the inside of the reaction vessel.
  • the temperature for crystallisation of compound (I) or a pharmaceutically acceptable salt thereof is typically from about 0 to about 100°C, preferably from about 5°C to about 75°C.
  • Precipitated crystals can be collected by filtration, centrifugation or decantation methods. Isolated crystals may be washed with an appropriate solvent.
  • Isolated crystals are typically dried at a temperature of from about 10 to about 100°C, preferably from about 30 to about 50°C, until the weight of the crystals becomes constant, if necessary, in the presence of a drying agent such as silica gel or calcium chloride and optionally under reduced pressure.
  • a drying agent such as silica gel or calcium chloride and optionally under reduced pressure.
  • Dried crystals may absorb water under conditions of about 20 to 90% relative humidity at temperatures of from about 10 to about 30°C, preferably about 50 to about 80% relative humidity at temperatures of from about 20 about 30°C, until the weight of the crystalline form becomes constant.
  • Crystals obtained in accordance with the invention can be further purified by recrystallisation or slurry purification. Recrystallisation may be accomplished by techniques familiar to those skilled in the art, including the following methods:
  • Cooling method compound (I), or a pharmaceutically acceptable salt thereof, is dissolved in a hot solvent and the resulting solution is cooled;
  • Precipitation method a solvent in which compound (I) or a pharmaceutically acceptable salt thereof is slightly soluble is added to a solution of compound (I) or a pharmaceutically acceptable salt thereof in a solvent in which compound (I) or a pharmaceutically acceptable salt thereof is readily soluble.
  • Slurry purification typically comprises stirring a suspension of compound (I), or a pharmaceutically acceptable salt thereof, in an appropriate solvent.
  • Solvents employed in the preparation of crystalline forms of compound (I) include ICH class 2 or preferably class 3 solvents.
  • esters such as ethyl acetate, alcohols such as ethanol, ketones such as methyl ethyl ketone, ethers such as methyl t-butyl ether, alkanes such as heptane, and water.
  • These solvents may be used singly or as mixtures.
  • Preferred solvents include IMS, acetonitrile, tetralin, cumene, 3-methyl-1- butanol, ethanol, methanol, isopropanol, ethyl acetate, methyl acetate, isopropyl acetate, water, heptane, TBME, THF, MEK, methyl isobutyl ketone, nPrOH and nBuOAc.
  • the present invention encompasses individual crystalline forms as defined above, and mixtures thereof with one or more other crystalline forms.
  • Crystalline Free Base of Compound (I) (Form A)
  • One preferred embodiment of the invention relates to the crystalline form of the free base of compound (I).
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 7.53 ⁇ 0.2, 9.60 ⁇ 0.2, 10.22 ⁇ 0.2, 11.29 ⁇ 0.2, 1 1.66 ⁇ 0.2, 12.26 ⁇ 0.2, 12.62 ⁇ 0.2, 13.17 ⁇ 0.2, 14.06 ⁇ 0.2, 14.85 ⁇ 0.2, 15.15 ⁇ 0.2, 15.57 ⁇ 0.2, 16.99 ⁇ 0.2, 17.68 ⁇ 0.2, 18.30 ⁇ 0.2, 18.39 ⁇ 0.2, 18.63 ⁇ 0.2, 18.97 ⁇ 0.2, 19.32 ⁇ 0.2 and 20.20 ⁇ 0.2.
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. Even more preferably, the crystalline form is characterized by having at least 7, 8, 9, 10, 11 , 12, 13, 14, 15, 16, 17 18 or 19 or more of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 7.53 ⁇ 0.2, 12.26 ⁇ 0.2, 14.06 ⁇ 0.2, 14.85 ⁇ 0.2 and 15.57 ⁇ 0.2. More preferably, the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. In one highly preferred embodiment, the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 5 or listed in Table 1.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak at a temperature between about 130°C and about 140°C, more preferably between about 132°C and about 138°C, even more preferably, between about 135°C and about 138°C, more preferably still, between about 136°C and about 138°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 6.
  • a further aspect of the invention relates to a process of preparing free base compound (I) in crystalline form, said process comprising crystallising amorphous compound (I) in free base form from methyl t-butyl ether (MTBE).
  • MTBE methyl t-butyl ether
  • the crystalline form of the free base is obtained from a supersaturated solution.
  • the process comprises heating compound (I) in MTBE to reflux, allowing the mixture to cool to room temperature, filtering the solid so formed, washing the solid with MTBE and drying under vacuum. More preferably, after refluxing, the reaction mixture is held for a period of 1 to 3 hours at a temperature below reflux (for example, 45-50°C) before being allowed to cool to room temperature.
  • a temperature below reflux for example, 45-50°C
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • Crystalline Citrate Salt (Form F)
  • the crystalline form is a citrate salt of compound (I).
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 5.14 ⁇ 0.2, 7.73 ⁇ 0.2, 10.24 ⁇ 0.2, 12.70 ⁇ 0.2, 13.06 ⁇ 0.2, 14.42 ⁇ 0.2, 15.30 ⁇ 0.2, 15.98 ⁇ 0.2, 16.74 ⁇ 0.2, 17.24 ⁇ 0.2, 18.05 ⁇ 0.2, 19.04 ⁇ 0.2, 20.23 ⁇ 0.2, 21.04 ⁇ 0.2, 22.45 ⁇ 0.2, 22.75 ⁇ 0.2, 24.01 ⁇ 0.2, 25.43 ⁇ 0.2, 26.51 ⁇ 0.2, 27.48 ⁇ 0.2, 28.77 ⁇ 0.2 and 29.71 ⁇ 0.2 [Form F].
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. Even more preferably, the crystalline form is characterized by having at least 7, 8, 9, 10, 1 1, 12, 13, 14, 15, 16, 17, 18, 19, 20 or 21 or more of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 17.24 ⁇ 0.2, 18.05 ⁇ 0.2, 19.04 ⁇ 0.2, 22.45 ⁇ 0.2, 22.75 ⁇ 0.2, 24.01 ⁇ 0.2 and 25.43 ⁇ 0.2 [Form F. More preferably, the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. Even more preferably, the crystalline form is characterized by having 6 or 7 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 7 or listed in Table 3.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows maximum endothermic peaks at a temperature between about 145°C and about 155°C and between about 165°C and about 200°C.
  • the crystalline form is characterized by a first maximum endothermic peak at a temperature between about 146°C and about 152°C, more preferably between about 147°C and about 151°C, and a broader second maximum endothermic peak between about 170°C and about 195°C, more preferably between about 175°C and about 190°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 8.
  • the crystalline form of the citrate salt of compound (I) is obtained from a supersaturated solution.
  • the invention relates to a process for preparing the citrate salt of compound (I) in crystalline form, said process comprising crystallizing the citrate salt from ethyl acetate.
  • the invention relates to a process for preparing the citrate salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises stirring a mixture of compound (I) and citric acid in ethyl acetate at ambient temperature, subjecting the mixture to a heat/cool cycle (60°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours, filtering the solid so formed, washing the solid with ethyl acetate and drying under vacuum. More preferably, the mixture is stored in a shaker during the heat/cool cycle.
  • a heat/cool cycle 60°C/RT, 4 hours
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form is a phosphate salt.
  • the crystalline phosphate salt exists in at least two different forms, depending on the solvent used for crystallisation.
  • each of these two different forms exist in hydrated and anhydrous forms, thereby giving rise to at least four different crystalline forms.
  • the two forms are designated Forms B and C.
  • the phosphate salt is crystallised from propan-2-ol (Form B). In another preferred embodiment, the phosphate salt is crystallised from ethanol (Form C).
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.46 ⁇ 0.2, 8.88 ⁇ 0.2, 9.67 ⁇ 0.2, 10.47 ⁇ 0.2, 12.78 ⁇ 0.2, 15.33 ⁇ 0.2, 16.12 ⁇ 0.2, 16.82 ⁇ 0.2, 18.13 ⁇ 0.2, 19.38 ⁇ 0.2, 19.95 ⁇ 0.2, 20.97 ⁇ 0.2, 24.11 ⁇ 0.2, 24.83 ⁇ 0.2, 26.54 ⁇ 0.2 and 28.11 ⁇ 0.2 [Form B].
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 7, 8, 9, 10, 11 , 12, 13, 14 or 15 or more of the aforementioned diffraction peaks. Preferably, the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 6.46 ⁇ 0.2, 16.12 + 0.2, 18.13 ⁇ 0.2, 19.38 ⁇ 0.2, 19.95 ⁇ 0.2, 20.97 ⁇ 0.2, 24.1 1 ⁇ 0.2 and 24.83 ⁇ 0.2 [Form B]. More preferably, the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 6, 7 or 8 of the aforementioned diffraction peaks
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 11 or listed in Table 6.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows maximum endothermic peaks at a temperature between about 65°C and about 90°C and between about 114°C and about 130°C.
  • the crystalline form is characterized by a first maximum endothermic peak at a temperature between about 70 °C and about 88°C, more preferably, between about 75°C and about 85°C.
  • the crystalline form is characterized by a second maximum endothermic peak at a temperature between about 1 18°C and about 125°C, more preferably, between about 120°C and about 125°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 12.
  • the present invention encompasses the crystalline phosphate salts in anhydrous and hydrated forms.
  • the crystalline form of the phosphate salt of compound (I) is obtained by precipitation.
  • the invention relates to a process for preparing the phosphate salt of compound (I) in crystalline form, said process comprising crystallizing the phosphate salt from a solution of propan-2-ol.
  • the invention relates to a process for preparing a crystalline phosphate salt of compound (I), said process comprising the steps of:
  • the process comprises adding a solution of phosphoric acid in water to a stirring solution of compound (I) in propan-2-ol at room temperature in a cool water bath. More preferably, the process comprises adding further propan-2-ol to the mixture and stirring for at least 1 hour before filtering the solid so formed, washing the solid with propan-2-ol and drying under vacuum. Preferably, the solid is isolated by vacuum filtration.
  • the solution of phosphoric acid in water is an 85 % solution (w w).
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from from 6.49 ⁇ 0.2, 8.91 ⁇ 0.2, 9.75 ⁇ 0.2, 10.52 ⁇ 0.2, 13.03 ⁇ 0.2, 15.44 ⁇ 0.2, 16.27 ⁇ 0.2, 17.85 ⁇ 0.2, 18.29 ⁇ 0.2, 19.52 ⁇ 0.2, 20.02 ⁇ 0.2, 21.11 ⁇ 0.2, 22.80 ⁇ 0.2, 24.92 ⁇ 0.2, 28.33 ⁇ 0.2 and 29.41 ⁇ 0.2 [Form C].
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 7, 8, 9, 10, 11 , 12, 13, 14 or 15 or more of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 6.49 ⁇ 0.2, 16.27 ⁇ 0.2, 18.29 ⁇ 0.2, 19.52 ⁇ 0.2, 20.02 ⁇ 0.2, 21.1 1 ⁇ 0.2, 22.80 ⁇ 0.2, 24.92 ⁇ 0.2 and 29.41 ⁇ 0.2 [Form C]. More preferably, the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 6, 7, 8 or 9 of the aforementioned diffraction peaks. In one highly preferred embodiment, the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 13 or listed in Table 5.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows maximum endothermic peaks at a temperature between about 66°C and about 90°C and between about 120°C and about 135°C.
  • the crystalline form is characterized by a first maximum endothermic peak at a temperature between about 70°C and about 88°C, more preferably, between about 80°C and about 87°C.
  • the crystalline form is characterized by a second maximum endothermic peak at a temperature between about 125°C and about 135°C, more preferably, between about 130°C and about 135°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 14.
  • the present invention encompasses the crystalline phosphate salts in anhydrous and hydrated forms.
  • the crystalline form of the phosphate salt of compound (I) is obtained by precipitation.
  • the invention relates to a process for preparing the phosphate salt of compound (I) in crystalline form, said process comprising crystallizing the phosphate salt from ethanol. More preferably, the invention relates to a process for preparing a crystalline phosphate salt of compound (I), said process comprising the steps of:
  • the process comprises adding a solution of phosphoric acid in water to a stirring solution of compound (I) in ethanol at room temperature in a cool water bath. More preferably, the process comprises further stirring the mixture at room temperature for at least 2 hours before filtering the solid so formed, washing the solid with ethanol and drying under vacuum.
  • the solid is isolated by vacuum filtration.
  • the solid is dried in a vacuum oven, for example, at a temperature of at least 40°C for at least 12, more preferably 24 hours.
  • the solution of phosphoric acid in water is an 85 % solution (w/w).
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form is a tartrate salt, more preferably, the L-tartrate salt.
  • the tartrate salt exists in at least two different forms, designated hereinafter as Form D and Form E.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 3.82 ⁇ 0.2, 7.57 ⁇ 0.2, 8.12 ⁇ 0.2, 10.53 ⁇ 0.2, 11.39 ⁇ 0.2, 12.00 ⁇ 0.2, 13.54 ⁇ 0.2, 15.15 ⁇ 0.2, 16.35 ⁇ 0.2, 16.88 ⁇ 0.2, 17.37 ⁇ 0.2, 18.51 ⁇ 0.2, 18.98 ⁇ 0.2, 19.77 ⁇ 0.2, 21.06 ⁇ 0.2, 22.70 ⁇ 0.2, 23.47 ⁇ 0.2, 24.66 ⁇ 0.2 and 28.73 ⁇ 0.2 [Form D].
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17 or 18 or more of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 3.82 ⁇ 0.2, 7.57 ⁇ 0.2, 15.15 ⁇ 0.2, 16.88 ⁇ 0.2, 19.77 ⁇ 0.2, 22.70 ⁇ 0.2, 23.47 ⁇ 0.2, 24.66 ⁇ 0.2 and 28.73 ⁇ 0.2 [Form D]. More preferably, the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 6, 7, 8 or 9 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 3 or listed in Table 2.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak at a temperature between about 145°C and about 154°C, more preferably between about 148°C and about 153°C, even more preferably, between about 150°C and about 152°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 4.
  • the crystalline form of the tartrate salt of compound (I) is obtained by precipitation.
  • the invention relates to a process for preparing the L- tartrate salt of compound (I) in crystalline form, said process comprising crystallizing the L-tartrate salt from a solution of ethyl acetate.
  • the invention relates to a process for preparing a crystalline form of the L-tartrate salt of compound (I), said process the steps of:
  • the process comprises stirring a mixture of L-tartaric acid, compound (I) and ethyl acetate under ambient conditions for at least 1 hour, more preferably, at least 2 hours, and isolating the precipitate so formed, washing with ethyl acetate and drying in a vacuum oven.
  • the precipitate is isolated by vacuum filtration.
  • the precipitate is dried at a temperature of at least 40°C for at least 12, more preferably 24 hours.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.67 ⁇ 0.2, 8.237 ⁇ 0.2, 9.777 ⁇ 0.2, 11.96 ⁇ 0.2, 12.38 ⁇ 0.2, 13.06 ⁇ 0.2, 13.38 ⁇ 0.2, 13.94 ⁇ 0.2, 14.90 ⁇ 0.2, 15.40 ⁇ 0.2, 15.95 ⁇ 0.2, 16.27 ⁇ 0.2, 16.54 ⁇ 0.2, 17.36 ⁇ 0.2, 17.57 ⁇ 0.2, 17.86 ⁇ 0.2, 19.64 + 0.2, 19.86 ⁇ 0.2, 20.12 ⁇ 0.2, 20.73 ⁇ 0.2, 21.14 ⁇ 0.2, 21.58 ⁇ 0.2, 22.57 ⁇ 0.2, 22.95 ⁇ 0.2, 23.29 ⁇ 0.2, 23.57 ⁇ 0.2, 24.07 ⁇ 0.2, 24.63 ⁇ 0.2, 25.30
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 7, 8, 9, 10....38 or more of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 6.67 ⁇ 0.2, 13.06 ⁇ 0.2, 13.38 ⁇ 0.2, 14.90 ⁇ 0.2, 17.36 ⁇ 0.2, 17.57 ⁇ 0.2, 19.64 ⁇ 0.2, 20.73 ⁇ 0.2, 23.57 ⁇ 0.2 and 25.30 ⁇ 0.2 (Form E). More preferably, the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 6, 7, 8, 9 or 10 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 1 or listed in Table 7.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak at a temperature between about 176°C and about 185°C, more preferably, between about 178°C and about 184°C, even more preferably, between about 180°C and about 183°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 2.
  • the Form E L-tartrate salt is obtained by recrystallising the Form D L-tartrate salt of compound (I) from a mixture of ethanol and acetonitrile
  • the invention relates to a process for preparing the L- tartrate salt (Form E) of compound (I) in crystalline form, said process comprising crystallizing the L-tartrate salt (Form D) from a mixture of ethanol and acetonitrile.
  • the L-tartrate salt (Form E) is recrystallized from a mixture of ethanol and acetonitrile.
  • one aspect of the invention relates to a process for preparing Form E L-tartrate salt of compound (I) in crystalline form, said process comprising the steps of:
  • step (iii) recrystallizing the crystalline L-tartrate salt (Form D) obtained in step (ii) from a mixture of ethanol and acetonitrile;
  • step (iii) comprises forming a suspension of the crystalline L-tartrate salt (Form D) obtained in step (ii) in ethanol and heating to at least 60°C, adding acetonitrile to the mixture and heating the mixture at reflux to form a solution.
  • the solution is then hot filtered and allowed to cool to room temperature, more preferably at a rate of about 5-10°C/hour.
  • the resulting suspension is then stirred for at least 12 hours at room temperature before filtering off the solid, washing with ethanol and drying.
  • the solid is dried in a vacuum oven at a temperature of at least 50°C for at least 12, more preferably 24 hours.
  • the ratio of ethanol to acetonitrile is from about 3:1 to about 10:1. More preferably, the ratio of ethanol to acetonitrile is 4:1 or 6:1. Even more preferably, the ratio of ethanol to acetonitrile is 4: 1 , 5: 1 or 6: 1.
  • the Form E L-tartrate salt is prepared from a slurry conversion of a mixture of Form D L-tartrate salt of compound (I) and Form E L-tartrate salt of compound (I).
  • Another aspect of the invention relates to a process for preparing Form E L-tartrate salt of compound (I) in crystalline form, said process comprising the steps of:
  • the slurry in step (iii) is a mixture of 50-99 % by weight of L-tartrate salt (Form D) and 1-50 by weight of % L-tartrate salt (Form E). More preferably, the slurry in step (iii) is a 50:50 mixture of L-tartrate salt (Form D) and L-tartrate salt (Form E).
  • the slurry is heated to a temperature of at least 40 °C, more preferably at least 45 °C for at least 24 hours, more preferably at least 48 hours, before isolating the solid by filtration, washing and drying under vacuum.
  • the Form E L-tartrate salt is obtained by recrystallising Form D L-tartrate salt from a mixture of ethanol and acetonitrile by seeding with one or more crystals of the Form E L-tartrate salt.
  • a process for preparing Form E L-tartrate salt which comprises recrystallizing Form D L-tartrate salt from a mixture of ethanol and acetonitrile, preferably with seeding using one or more crystals of the Form E L-tartrate salt.
  • the invention relates to a process for preparing Form E L-tartrate salt of compound (I) in crystalline form, said process comprising the steps of:
  • one aspect relates to a process for preparing Form E L-tartrate salt which comprises crystallizing Form E L-tartrate salt from a solution of ethyl acetate, preferably seeding with one or more crystals of the Form E L-tartrate salt.
  • the Form E L-tartrate salt is prepared from compound (I) in free base form.
  • the the Form E L-tartrate salt is obtained by treating compound (I) in free base form with a solution of tartaric acid in water/ethanol, and seeding the resulting mixture with a crystal of Form E L-tartrate salt obtained by any one of the methods described herein.
  • one particularly preferred embodiment of the invention relates to a process for preparing Form E L-tartrate salt of compound (I) in crystalline form, said process comprising the steps of:
  • step (ii) adding solution of tartaric acid in water/ethanol to the reaction mixture obtained in step (i);
  • step (iv) isolating crystalline L-tartrate salt (Form E) from the reaction mixture.
  • the reaction mixture formed in step (i) is heated at reflux.
  • the solution of tartaric acid in water/ethanol is added whilst maintaining the temperature at reflux.
  • step (ii) comprises polish filtering the reaction mixture before cooling to about 70°C.
  • the mixture is stirred at a temperature of at least 70°C for at least 1 hour before cooling to room temperature.
  • the mixture is then stirred for at least 1 hour, more preferably at least 2 hours, before filtering.
  • the product obtained in the filtration step is washed with ethanol and dried.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above processes.
  • the crystalline form is a benzenesulfonate salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 5.72 ⁇ 0.2, 11.45 ⁇ 0.2, 11.79 ⁇ 0.2, 15.56 ⁇ 0.2, 16.57 ⁇ 0.2, 18.04 ⁇ 0.2, 19.14 ⁇ 0.2, 20.02 ⁇ 0.2, 21.05 ⁇ 0.2, 22.80 ⁇ 0.2, 23.16 ⁇ 0.2, 24.44 ⁇ 0.2, 25.40 ⁇ 0.2 and 28.74 ⁇ 0.2 [Form G].
  • the crystalline form is characterized by having three or more, four or more, five or more, or six or more of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 7, 8, 9, 10, 1 1 , 12 or 13 or more of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by an x-ray powder diffraction pattern comprising two or more diffraction peaks at 2[theta] values selected from 15.56 ⁇ 0.2, 16.57 ⁇ 0.2, 18.04 ⁇ 0.2, 20.02 ⁇ 0.2, 21.05 ⁇ 0.2, 22.80 ⁇ 0.2, 23.16 ⁇ 0.2 and 24.44 ⁇ 0.2 [Form G].
  • the crystalline form is characterized by having three, four or five of the aforementioned diffraction peaks. More preferably, the crystalline form is characterized by having 6, 7, 8, 9, 10, 1 1 , 12, 13 or 14 of the aforementioned diffraction peaks. In one highly preferred embodiment, the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 9 or listed in Table 4.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak at a temperature between about 145°C and about 155°C, more preferably, between about 146°C and about 154°C, even more preferably, between about 1 7°C and about 154°C.
  • the crystalline form is characterized by a differential scanning calorimetry trace substantially in accordance with that shown in Figure 10.
  • the crystalline form of the benzenesuifonic acid salt of compound (I) is obtained from a supersaturated solution.
  • the invention relates to a process for preparing the benzenesuifonic acid salt of compound (I) in crystalline form, said process comprising crystallizing the benzenesuifonic acid salt from a solution of methyl t-butyl ether (MTBE).
  • MTBE methyl t-butyl ether
  • the invention relates to a process for preparing the benzenesuifonic acid salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises stirring a mixture of compound (I) and benzenesuifonic acid in MTBE at ambient temperature for at least 24 hours.
  • the mixture is then subjected to a heat/cool cycle (60°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours, filtering the solid so formed, washing the solid with MTBE and drying under vacuum.
  • a heat/cool cycle 60°C/RT, 4 hours
  • the mixture is stored in a shaker during the heat/cool cycle.
  • the crystalline form of compound (I) is a hydrochloride salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 5.6 ⁇ 0.2, 8.6 ⁇ 0.2, 9.5 ⁇ 0.2, 10.9 ⁇ 0.2, 11.2 ⁇ 0.2, 12.7 ⁇ 0.2, 13.0 ⁇ 0.2, 14.3 ⁇ 0.2, 16.0 ⁇ 0.2, 17.3 ⁇ 0.2, 17.7 ⁇ 0.2, 18.8 ⁇ 0.2, 19.1 ⁇ 0.2, 20.3 ⁇ 0.2, 20.7 ⁇ 0.2, 22.9 ⁇ 0.2, 23.6 ⁇ 0.2, 24.5 ⁇ 0.2, 25.0 ⁇ 0.2, 25.5 ⁇ 0.2, 25.8 ⁇ 0.2, 26.4 ⁇ 0.2 and 29.1 ⁇ 0.2 [Form H]. More preferably, the crystalline form is characterized by having 1 , 2, 3, 4.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 19 or listed in Table 8.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows endothermic peaks at temperatures with onset at about 51°C, about 84°C, about 97°C and about 144°C.
  • the invention relates to a process for preparing the hydrochloride salt (Form H) of compound (I) in crystalline form, said process comprising crystallizing the hydrochloride salt (Form H) from methyl t-butyl ether (MTBE).
  • a further aspect of the invention relates to a process for preparing the hydrochloric acid salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises agitating a mixture of compound (I) and hydrochloric acid in MTBE at ambient temperature.
  • the mixture is then subjected to a heat/cool cycle (40°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours, filtering the solid so formed, washing the solid with MTBE and drying under vacuum.
  • the mixture is stored in a shaker during the heat/cool cycle.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of the hydrochloride salt is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 4.9 ⁇ 0.2, 6.4 ⁇ 0.2, 7.5 ⁇ 0.2, 12.1 ⁇ 0.2, 14.4 ⁇ 0.2, 19.8 ⁇ 0.2, 21.5 ⁇ 0.2, 23.4 ⁇ 0.2 and 25.7 ⁇ 0.2 [Form I]. More preferably, the crystalline form is characterized by having 1 , 2, 3, 4, 5, 6, 7, 8 or 9 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 20 or listed in Table 9.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows endothermic peaks with onset temperatures at about 98°C and about 130°C.
  • the invention relates to a process for preparing the hydrochloride salt (Form I) of compound (I) in crystalline form, said process comprising crystallizing the hydrochloride salt (Form I) from ethyl acetate.
  • a further aspect of the invention relates to a process for preparing the hydrochloric acid salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises agitating a mixture of compound (I) and hydrochloric acid in ethyl acetate at ambient temperature.
  • the mixture is then subjected to a heat/cool cycle (40°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours.
  • the solid so formed is filtered, washed with ethyl acetate and dried under vacuum. More preferably, the mixture is stored in a shaker during the heat/cool cycle.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of compound (I) is a hydrobromide salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.4 ⁇ 0.2, 7.2 ⁇ 0.2, 12.0 ⁇ 0.2, 14.4 ⁇ 0.2, 17.1 ⁇ 0.2, 19.6 ⁇ 0.2, 21.4 ⁇ 0.2 and 25.5 ⁇ 0.2 [Form J]. ore preferably, the crystalline form is characterized by having 1 , 2, 3, 4, 5, 6, 7 or 8 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 21 or listed in Table 10.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak with an onset at a temperature of about 138°C.
  • the invention relates to a process for preparing the hydrobromic acid salt (Form J) of compound (I) in crystalline form, said process comprising crystallizing the hydrobromic acid (Form J) salt from ethyl acetate.
  • a further aspect of the invention relates to a process for preparing the hydrobromic acid salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises agitating a mixture of compound (I) and hydrobromic acid in ethyl acetate at ambient temperature.
  • the mixture is then subjected to a heat/cool cycle (40°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours.
  • the solid so formed is filtered, washed with ethyl acetate and dried under vacuum. More preferably, the mixture is stored in a shaker during the heat/cool cycle.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of compound (I) is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows maximum endothermic peak at temperatures of about 51 °C and 90°C.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 5.7 ⁇ 0.2, 16.4 ⁇ 0.2, 17.7 ⁇ 0.2, 18.4 ⁇ 0.2, 19.6 ⁇ 0.2, 20.5 ⁇ 0.2, 24.1 ⁇ 0.2, 25.3 ⁇ 0.2, 26.0 ⁇ 0.2 and 28.1 ⁇ 0.2 [Form K]. More preferably, the crystalline form is characterized by having 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 28 or listed in Table 17.
  • the crystalline form is characterized by a DSC/TGA trace substantially in accordance with Figure 29.
  • a further aspect of the invention relates to a process for preparing the hydrobromic acid salt of compound (I) (Form K) in crystalline form which comprises subjecting the Form J hydrobromic acid salt to a temperature of at least 40°C at a relative humidity of at least 75% for 7 days. More preferably, the invention relates to a process for preparing the hydrobromic acid salt of compound (I) (form K) in crystalline form, said process comprising the steps of:
  • step (iii) comprises storing the crystalline hydrobromic acid salt (form J) for an extended period, more preferably, for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours, even more preferably for at least 7 days.
  • the crystalline product is then filtered, washed and dried under vacuum.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above processes.
  • the crystalline form of compound (I) is a mesylate salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.3 ⁇ 0.2, 7.9 ⁇ 0.2, 12.5 ⁇ 0.2, 13.4 ⁇ 0.2, 14.6 ⁇ 0.2, 15.9 ⁇ 0.2, 16.5 ⁇ 0.2, 17.5 ⁇ 0.2, 18.1 ⁇ 0.2, 18.7 ⁇ 0.2, 19.3 ⁇ 0.2, 20.0 ⁇ 0.2, 20.6 ⁇ 0.2, 20.9 ⁇ 0.2, 21.7 ⁇ 0.2, 22.6 ⁇ 0.2, 23.8 ⁇ 0.2, 24.5 ⁇ 0.2, 25.1 ⁇ 0.2, 25.5 ⁇ 0.2, 26.1 ⁇ 0.2, 27.5 ⁇ 0.2, 29.1 ⁇ 0.2, 29.7 ⁇ 0.2 and 30.3 ⁇ 0.2 [Form L].
  • the crystalline form is characterized by having 1 , 2, 3, 4, 5 25 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 22 or listed in Table 1.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak with an onset temperature of about 126°C.
  • the crystalline form is characterized by a DSC/TGA trace substantially in accordance with Figure 30.
  • the invention relates to a process for preparing the mesylate salt of compound (I) in crystalline form, said process comprising crystallizing the mesylate salt from TBME. More preferably, the invention relates to a process for preparing the mesylate salt of compound (I) in crystalline form, said process comprising the steps of: (i) preparing a reaction mixture comprising compound (I) in free base form, methanesulfonic acid and TB E; and
  • the process comprises agitating a mixture of compound (I) and methanesulfonic acid in TBME at ambient temperature for at least 12 hours, more preferably at least 16 hours, or at least 24 hours.
  • the mixture is then heated to at least 40°C and stirred for at least 1 hour, before cooling to room temperature and stirring for at least 12 hours.
  • THF is added to the mixture and stirring continued for at least a further 2 hours.
  • the mixture is then subjected to a heat/cool cycle (40°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours.
  • TBME is added to the mixture and the resulting solid filtered, washed with TBME and dried under vacuum. More preferably, the mixture is stored in a shaker during the heat/cool cycle.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of compound (I) is a maleate salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 3.8 ⁇ 0.2, 7.6 ⁇ 0.2, 8.5 ⁇ 0.2, 10.8 ⁇ 0.2, 11.4 ⁇ 0.2, 12.2 ⁇ 0.2, 15.2 ⁇ 0.2, 15.8 ⁇ 0.2, 17.0 ⁇ 0.2, 18.0 ⁇ 0.2, 18.8 ⁇ 0.2, 19.4 ⁇ 0.2, 20.3 ⁇ 0.2, 21.6 ⁇ 0.2, 22.6 ⁇ 0.2, 23.6 ⁇ 0.2, 24.3 ⁇ 0.2, 24.8 ⁇ 0.2, 26.0 ⁇ 0.2, 27.2 ⁇ 0.2, 27.9 ⁇ 0.2, 28.2 ⁇ 0.2, 28.8 ⁇ 0.2, 29.9 ⁇ 0.2, 30.2 ⁇ 0.2, 31.7 ⁇ 0.2, 32.7 ⁇ 0.2 and 33.2 ⁇ 0.2 [Form M].
  • the crystalline form is characterized by having 1 , 2, 3, 4, 5, 6 or 28 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 23 or listed in Table 12.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows maximum endothermic peak at an onset temperature of about 116 °C.
  • the crystalline form is characterized by a DSC/TGA trace substantially in accordance with Figure 31.
  • the invention relates to a process for preparing the maleate salt of compound (I) in crystalline form, said process comprising crystallizing the maleate salt from TBME.
  • the invention relates to a process for preparing the maleate salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises agitating a mixture of compound (I) and maleic acid in TBME at ambient temperature for at least 12 hours, more preferably, at least 16 hours.
  • the solid so formed is filtered, washed with TBME and dried under vacuum. More preferably, the mixture is stored in a shaker during the heat/cool cycle.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of compound (I) is a gentisate salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.32 ⁇ 0.2, 12.16 ⁇ 0.2, 12.45 ⁇ 0.2, 13.13 ⁇ 0.2, 14.41 ⁇ 0.2, 14.83 ⁇ 0.2, 16.37 ⁇ 0.2, 17.12 ⁇ 0.2, 18.79 ⁇ 0.2, 19.49 ⁇ 0.2, 20.42 ⁇ 0.2, 23.37 ⁇ 0.2 and 23.77 ⁇ 0.2 [Form O]. More preferably, the crystalline form is characterized by having 1 , 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 , 12 or 13 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 24 or listed in Table 13.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak with an onset at a temperature of about 92°C.
  • the crystalline form is characterized by a DSC/TGA trace substantially in accordance with Figure 32.
  • the invention relates to a process for preparing the gentisate salt of compound (I) in crystalline form, said process comprising crystallizing the gentisate salt from acetonitrile.
  • the invention relates to a process for preparing the gentisate salt of compound (I) in crystalline form (form O), said process comprising the steps of:
  • step (iii) crystallising the gentisate salt formed in step (ii) from acetonitrile.
  • the process comprises agitating a mixture of compound (I) and gentisic acid in ethyl acetate at ambient temperature.
  • the mixture is then subjected to a heat/cool cycle (40°C/RT, 4 hours) for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours. More preferably, the mixture is stored in a shaker during the heat/cool cycle.
  • the mixture is then cooled to about 5 °C for at least 24 hours, and then to about -18°C for at least 24 hours.
  • the gentisate salt formed in step (ii) is dried under vacuum and then crystallised from acetonitrile.
  • acetonitrile is added to the gentisate salt formed in step (ii) and the mixture stored in a shaker at about 26°C for at least 6 hours.
  • the mixture is then cooled to 5°C for at least 12 or 16 hours, and then cooled to -18°C for at least 24 hours.
  • the crystalline gentisate salt of formula (I) is obtained by slow evaporation of the acetonitrile.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of compound (I) is a fumarate salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 3.8 ⁇ 0.2, 7.7 ⁇ 0.2, 8.1 ⁇ 0.2, 8.8 ⁇ 0.2, 10.2 ⁇ 0.2, 11.3 ⁇ 0.2, 13.1 ⁇ 0.2, 15.2 ⁇ 0.2, 15.5 ⁇ 0.2, 16.5 ⁇ 0.2, 17.7 ⁇ 0.2, 19.1 ⁇ 0.2, 19.6 ⁇ 0.2, 20.0 ⁇ 0.2, 20.9 ⁇ 0.2, 21.5 ⁇ 0.2, 21.9 ⁇ 0.2, 22.7 ⁇ 0.2, 23.2 ⁇ 0.2, 23.8 ⁇ 0.2, 24.1 ⁇ 0.2, 25.0 ⁇ 0.2, 25.3 ⁇ 0.2, 26.7 ⁇ 0.2, 27.9 ⁇ 0.2 and 28.9 ⁇ 0.2 [Form P]. More
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 25 or listed in Table 14.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak with an onset at a temperature of about 140°C.
  • the crystalline form is characterized by a DSC TGA trace substantially in accordance with Figure 33.
  • the invention relates to a process for preparing the fumarate salt of compound (I) in crystalline form, said process comprising crystallizing the fumarate salt from ethyl acetate.
  • a further aspect of the invention relates to a process for preparing the fumarate salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises agitating a mixture of compound (I) and fumaric acid in ethyl acetate at ambient temperature and agitating for at least 12 hours, more preferably a least 16 hours.
  • the solid so formed is filtered, washed with ethyl acetate and dried under vacuum.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form of compound (I) is a L-malate salt.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.7 ⁇ 0.2, 8.6 ⁇ 0.2, 9.3 ⁇ 0.2, 11.0 ⁇ 0.2, 12.7 ⁇ 0.2, 13.6 ⁇ 0.2, 14.1 ⁇ 0.2, 15.1 ⁇ 0.2, 15.8 ⁇ 0.2, 16.5 ⁇ 0.2, 17.8 ⁇ 0.2, 18.7 ⁇ 0.2, 19.5 ⁇ 0.2, 19.8 ⁇ 0.2, 21.2 ⁇ 0.2, 22.5 ⁇ 0.2, 23.5 ⁇ 0.2, 24.9 ⁇ 0.2 and 25.7 ⁇ 0.2 [Form Q]. More preferably, the crystalline form is characterized by having 1 , 2, 3, 4, 5, 6, 7....or 19 of the aforementioned diffraction peaks.
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 26 or listed in Table 15.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak with an onset at a temperature of about 81 °C.
  • the crystalline form is characterized by a DSC TGA trace substantially in accordance with Figure 34.
  • the invention relates to a process for preparing the L- malate salt of compound (I) in crystalline form, said process comprising crystallizing the L-malate salt from ethyl acetate.
  • a further aspect of the invention relates to a process for preparing the L-malate salt of compound (I) in crystalline form, said process comprising the steps of:
  • the process comprises agitating a mixture of compound (I) and L-malic acid in ethyl acetate at ambient temperature for at least 24 hours.
  • the mixture is then heated to a temperature of about 40°C and stirred for at least 1 hour, before cooling to room temperature and stirring for at least 12 hours.
  • the mixture is then cooled to about 5°C for at least 72 hours, before cooling to about -18°C for at least 30 hours.
  • the mixture is stirred at room temperature for 1 hour before filtering the solid so formed, washing with ethyl acetate and drying under vacuum.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • the crystalline form is characterized by an x-ray powder diffraction pattern having two or more diffraction peaks at 2[theta] values selected from 6.77 ⁇ 0.2, 9.85 ⁇ 0.2, 12.19 ⁇ 0.2, 13.36 ⁇ 0.2, 13.59 ⁇ 0.2, 14.15 ⁇ 0.2, 15.88 ⁇ 0.2, 16.44 ⁇ 0.2, 17.33 ⁇ 0.2, 17.75 ⁇ 0.2, 19.73 ⁇ 0.2, 20.1 ⁇ 0.2, 20.50 ⁇ 0.2, 20.84 ⁇ 0.2, 21.30 ⁇ 0.2, 22.23 ⁇ 0.2, 23.27 ⁇ 0.2, 23.83 ⁇ 0.2, 24.19 ⁇ 0.2, 24.61 ⁇ 0.2, 25.18 ⁇ 0.2, 25.67 ⁇ 0.2, 26.03 ⁇ 0.2, 26.31 ⁇ 0.2, 26.91 ⁇ 0.2, 27.78 ⁇ 0.2, 28.76 ⁇ 0.2, 31.11 ⁇ 0.2
  • the crystalline form is characterized by an x-ray powder diffraction pattern in which the peak positions are substantially in accordance with the peak positions of the pattern shown in Figure 27 or listed in Table 16.
  • the crystalline form is characterized by a differential scanning calorimetry trace recorded at a heating rate of 20°C per minute which shows a maximum endothermic peak with an onset at a temperature of about 104°C.
  • the crystalline form is characterized by a DSC/TGA trace substantially in accordance with Figure 35.
  • the invention relates to a process for preparing the L- malate salt (Form R) of compound (I) in crystalline form, said process comprising subjecting L-malate salt (Form Q) to a temperature of at least 40°C and a relative humidity of at least 75% for 7 days.
  • the invention relates to a process for preparing the L-malate salt of compound (I) (form R) in crystalline form, said process comprising the steps of: (i) preparing a reaction mixture comprising compound (I) in free base form, L-malic acid and ethyl acetate;
  • step (iii) comprises storing the crystalline hydrobromic acid salt (form J) for an extended period, more preferably, for at least 24 hours, more preferably, 48 hours, even more preferably 72 hours, more preferably for at least 7 days.
  • the crystalline product is then filtered, washed and dried under vacuum.
  • Another aspect of the invention relates to a product obtainable by, or obtained by, the above process.
  • Compound (I) has shown to exhibit potent inhibitory activity on cyclin dependent kinases, regulating proliferation, transcription and cytoskeletal organization and is therefore believed to be of use in the treatment of proliferative disorders (such as cancer and alopecia), immune-mediated and inflammatory disorders (such as graft-versus-host disease (GvHD), transplant rejection and psoriasis), autoimmune and autoimmune- mediated disorders (such as Hashimoto's thyroiditis, pernicious anemia, Addison's disease, type I diabetes, rheumatoid arthritis, systemic lupus erythematosus, dermatomyositis, Sjogren's syndrome, drug-induced lupus erythematosus, multiple scleroris, myasthenia gravis, Reiter's syndrome and Grave's disease, pemphigus vulgaris), kidney disorders (such as glomerulonephritis and polycystic kidney disease), cardiovascular disorders (such as restenos
  • Another aspect of the invention relates to the use of a crystalline form as described above in the preparation of a medicament for the prevention or treatment of a proliferative disorder.
  • Another aspect of the invention relates to a method for the prevention or treatment of a proliferative disorder, said method comprising administering a pharmacologically effective amount of a crystalline form as described above to a subject in need thereof.
  • the subject is a warm blooded animal, more preferably still, a human.
  • preparation of a medicament includes the use of one or more of the above described forms directly as the medicament in addition to their use in a screening programme for further antiproliferative agents or in any stage of the manufacture of such a medicament.
  • an anti-proliferative effect within the scope of the present invention may be demonstrated by the ability to inhibit cell proliferation in an in vitro whole cell assay. Using such assays it may be determined whether a compound is antiproliferative in the context of the present invention.
  • the proliferative disorder is a cancer or leukaemia.
  • the term proliferative disorder is used herein in a broad sense to include any disorder that requires control of the cell cycle, for example cardiovascular disorders such as restenosis and cardiomyopathy, genetic proliferative diseases such as polycystic kidney disease,
  • the proliferative disorder is a solid tumour.
  • the proliferative disorder is a haematological cancer.
  • the haematological cancer is leukaemia, more preferably, advanced leukaemias or myelodysplasia syndromes (MDS).
  • MDS myelodysplasia syndromes
  • Other examples include acute myelogenous leukaemia (AML), acute lymphocytic leukaemia (ALL) or chronic lymphocytic leukaemia (CLL).
  • the proliferative disorder is selected from glomerulonephritis, rheumatoid arthritis, psoriasis and chronic obstructive pulmonary disorder.
  • the compounds of the invention are also useful in the preparation of medicaments for the treatment of various ophthalmic disorders.
  • the ophthalmic disorder is glaucoma, exudative age-related macular degeneration (AMD) or proliferative diabetic retinopathy (PDR).
  • ALD exudative age-related macular degeneration
  • PDR
  • the crystalline form When crystalline forms of the invention are used as a medicament, preferably as an agent for treatment or prevention of proliferative disorders, the crystalline form can be administered alone, or as a mixture of the crystalline form with an appropriate pharmacologically acceptable excipient(s), and/or diluent(s) and/or carrier(s).
  • compositions according to the present invention can be in unit dosage form such as tablets, capsules, granules, powders, syrups, injections, ointments, solutions, suspensions, aerosols, troches or the like for oral, topical (e.g. for psoriasis) or parenteral administration.
  • the choice of pharmaceutical carrier, excipient or diluent can be selected with regard to the intended route of administration and standard pharmaceutical practice.
  • the pharmaceutical compositions may comprise as, or in addition to, the carrier, excipient or diluent any suitable binder(s), lubricant(s), suspending agent(s), coating agent(s), solubilising agent(s).
  • the pharmaceutical compositions may be for human or animal usage in human and veterinary medicine.
  • the pharmaceutical compositions can be prepared in a known manner by using additives such as excipients, binding agents, disintegrating agents, lubricating agents, stabilizing agents, corrigents, suspending agents, diluents and solvents.
  • additives such as excipients, binding agents, disintegrating agents, lubricating agents, stabilizing agents, corrigents, suspending agents, diluents and solvents.
  • an excipient includes a sugar derivative such as lactose, sucrose, glucose, mannitol, or sorbitol; a starch derivative such as corn starch, potato starch, alpha -starch, dextrin, carboxy methylstarch; a cellulose derivative such as crystalline cellulose, low-substituted hydroxypropylcellulose, hydroxypropylmethylcellulose, carboxymethyl-cellulose, calcium carboxymethylcellulose, internal-cross-linked sodium carboxymethylcellulose; acacia; dextran; pullulan; a silicate derivative such as light silicic acid anhydride, synthetic aluminum silicate, magnesium aluminate metasilicate; a phosphate derivative such as calcium phosphate; a carbonate derivative such as calcium carbonate; a sulfate derivative such as calcium sulfate; or the like.
  • a sugar derivative such as lactose, sucrose, glucose, mannitol, or sorbitol
  • a starch derivative such as
  • Acceptable carriers or diluents for therapeutic use are well known in the pharmaceutical art, and are described, for example, in Remington's Pharmaceutical Sciences, Mack Publishing Co. (A. R. Gennaro edit. 1985).
  • suitable carriers include lactose, starch, glucose, methyl cellulose, magnesium stearate, mannitol, sorbitol and the like.
  • suitable diluents include ethanol, glycerol and water.
  • An example of a disintegrating agent includes an excipient described hereinbefore, a chemically modified starch or cellulose derivative such as sodium cross-carmellose, sodium carboxymethylstarch, cross-linked polyvinylpyrrolidone or the like.
  • Preservatives, stabilizers, dyes and even flavoring agents may be provided in the pharmaceutical composition.
  • preservatives include sodium benzoate, sorbic acid and esters of p-hydroxybenzoic acid.
  • Antioxidants and suspending agents may be also used.
  • An example of a stabilizing agent includes a para-hydroxybenzoic acid ester derivative such as methylparabene, propylparabene; an alcohol derivative such as chlorobutanol, benzyl alcohol, phenetyl alcohol; benzalkonium chloride; a phenol derivative such as phenol, cresol; thimerosal; acetic anhydride; sorbic acid; or the like.
  • An example of a corrigent includes a sweetning, souring, and flavoring agents or the like all of which are ordinarily used.
  • An example of a solvent includes water, ethanol, glycerin or the like.
  • Suitable binders include an excipient described hereinbefore; gelatin; polyvinylpyrrolidone; macrogol; or the like, starch, natural sugars such as glucose, anhydrous lactose, free-flow lactose, beta-lactose, corn sweeteners, natural and synthetic gums, such as acacia, tragacanth or sodium alginate, carboxymethyl cellulose and polyethylene glycol.
  • An example of a lubricating agent includes talc; stearic acid; a metal stearate derivative such as calcium stearate, magnesium stearate, sodium stearate; colloidal silica; veegum; a wax such as beeswax or spermaceti; boric acid; a glycol; a carboxy acid derivative such as fumaric acid, adipic acid; a sodium carboxylate such as sodium benzoate; a sulfate such as sodium sulfate; leucine; a lauryl sulfate such as sodium lauryl sulfate, or magnesium lauryl sulfate; a silicic acid derivative such as silicic acid anhydride, silicic acid hydrate; a starch derivative described above as an excipient; sodium oleate, sodium acetate, sodium chloride, or the like.
  • compositions of the present invention may be adapted for oral, rectal, vaginal, parenteral, intramuscular, intraperitoneal, intraarterial, intrathecal, intrabronchial, subcutaneous, intradermal, intravenous, nasal, buccal or sublingual routes of administration.
  • compositions For oral administration, particular use is made of compressed tablets, pills, tablets, gellules, drops, and capsules. Preferably, these compositions contain from 1 to 250 mg and more preferably from 10-100 mg, of active ingredient per dose.
  • compositions of the present invention may also be in form of suppositories, pessaries, suspensions, emulsions, lotions, ointments, creams, gels, sprays, solutions or dusting powders.
  • transdermal administration is by use of a skin patch.
  • the active ingredient can be incorporated into a cream consisting of an aqueous emulsion of polyethylene glycols or liquid paraffin.
  • the active ingredient can also be incorporated, at a concentration of between 1 and 10% by weight, into an ointment consisting of a white wax or white soft paraffin base together with such stabilisers and preservatives as may be required.
  • Injectable forms may contain between 10 - 1000 mg, preferably between 10 - 250 mg, of active ingredient per dose.
  • compositions may be formulated in unit dosage form, i.e., in the form of discrete portions containing a unit dose, or a multiple or sub-unit of a unit dose.
  • the dose of the crystalline form of compound (I) will depend on such factors as symptom, body weight and age of the patient.
  • a suitable dosage level is 0.1 mg (preferably 1 mg) per day to 100 mg (preferably 50 mg) per day.
  • the crystalline form of the compound of formula (I) can be administered as either a single unit dosage, or if desired, the dosage may be divided into convenient subunits administered at one to several times throughout the day depending on the symptoms of the patient.
  • a person of ordinary skill in the art can easily determine an appropriate dose of one of the instant compositions to administer to a subject without undue experimentation.
  • a physician will determine the actual dosage which will be most suitable for an individual patient and it will depend on a variety of factors including the activity of the specific compound employed, the metabolic stability and length of action of that compound, the age, body weight, general health, sex, diet, mode and time of administration, rate of excretion, drug combination, the severity of the particular condition, and the individual undergoing therapy.
  • the dosages disclosed herein are exemplary of the average case. There can of course be individual instances where higher or lower dosage ranges are merited, and such are within the scope of this invention.
  • Figure 1 shows the X-ray powder diffraction pattern of Form E of the L-tartrate salt of compound (I), as obtained by Example 5.2.
  • the diffraction pattern was obtained by irradiation of the crystalline product using a PANalytical diffractometer.
  • Figure 2 is a DSC thermogram of Form E of the L-tartrate salt of compound (I) obtained using a PerkinElmer DSC4000 at a heating rate of 20°C.min ⁇ 1 . Peak max is observed at 182.40°C.
  • Figure 3 shows the X-ray powder diffraction pattern of Form D of the L-tartrate salt of compound (I) as obtained by Example 4.
  • the diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS C2 GADDS.
  • Figure 4 is a DSC thermogram of Form D of the L-tartrate salt of compound (I) as obtained by Example 4, using Mettler DSC823e at a heating rate of 20°C.min "1 . Peak max is observed at 151.83°C.
  • Figure 5 shows the X-ray powder diffraction pattern of crystalline free base (Form A) of compound (I) as obtained by Example 1.
  • the diffraction pattern was obtained by irradiation of the crystalline product using a PANalytical diffractometer.
  • Figure 6 shows a DSC thermogram (lower trace) of crystalline free base (Form A) of compound (I) as obtained by Example 1 , using a PerkinElmer Pyris 6 at a heating rate of 20°C.min "1 (peak max is observed at 137.63°C).
  • the upper trace shows TGA for the same salt measured using a Pyris 1 TGA at a heating rate of 20°C.min "1 . No significant mass loss was observed up to 250°C, onset observed at 369.39°C.
  • Figure 7 shows the X-ray powder diffraction pattern of the citrate salt (Form F) of compound (I) as obtained by Example 2.
  • the diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS C2 GADDS.
  • Figure 8 shows a DSC thermogram (lower trace) of the citrate salt (Form F) of compound (I) as obtained by Example 2, using Mettler DSC823e at a heating rate of 10 "C.rnin "1 (peak max observed at 150.83°C and 187.83).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851e at a heating rate of 10°C.min "
  • Figure 9 shows the X-ray powder diffraction pattern of the benzenesulfonic acid salt (Form G) of compound (I) as obtained by Example 3. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS C2 GADDS.
  • Figure 10 shows a DSC thermogram (lower trace) of the benzenesulfonic acid salt (Form G) of compound (I) as obtained by Example 3, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 153.00).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851e at a heating rate of 10°C.min "1 .
  • Figure 11 shows the X-ray powder diffraction pattern of the phosphate salt (Form B) of compound (I) as obtained by Example 7. The diffraction pattern was obtained by irradiation of the crystalline product Bruker AXS C2 GADDS.
  • Figure 12 is a DSC thermogram (lower trace) of Form 1 the phosphate salt (Form B) of compound (I) as obtained by Example 7, using Mettler DSC823e at a heating rate of 10°C.min '1 (peak max observed at 84.95 and 123.93).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851 e with a heating rate of 10°C.min '1 .
  • Figure 13 shows the X-ray powder diffraction pattern of the phosphate salt (Form C) of compound (I) as obtained by Example 6. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS C2 GADDS.
  • Figure 14 is a DSC thermogram of Form 2 of the phosphate salt (Form C) of compound (I) as obtained by Example 6, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 86.50 and 132.17).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851 e with a heating rate of 10°C.min "1 .
  • Figure 15 shows an isotherm plot for Form A (weight change % vs RH %) as measured using a Hiden Isochema moisture sorption analyser.
  • Figure 16 shows a kinetic plot of weight change (%) of Form A vs time and relative humidity %.
  • Figure 17 shows XRPD analysis of Form A post GVS.
  • Figure 18 shows XRPD analysis of Form A pre and post solubility study.
  • Figure 19 shows the X-ray powder diffraction pattern of the hydrochloride salt (Form H) of compound (I) as obtained by Example 8. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 20 shows the X-ray powder diffraction pattern of the hydrochloride salt (Form I) of compound (I) as obtained by Example 9.
  • the diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 21 shows the X-ray powder diffraction pattern of the hydrobromide salt (Form J) of compound (I) as obtained by Example 10. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 22 shows the X-ray powder diffraction pattern of the mesylate salt (Form L) of compound (I) as obtained by Example 12. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 23 shows the X-ray powder diffraction pattern of the maleate salt (Form M) of compound (I) as obtained by Example 13.
  • the diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 24 shows the X-ray powder diffraction pattern of the gentisate salt (Form O) of compound (I) as obtained by Example 15.
  • the diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 25 shows the X-ray powder diffraction pattern of the fumarate salt (Form P) of compound (I) as obtained by Example 16.
  • the diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 26 shows the X-ray powder diffraction pattern of the L-malate salt (Form Q) of compound (I) as obtained by Example 17. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 27 shows the X-ray powder diffraction pattern of the L-malate salt (Form R) of compound (I) as obtained by Example 18. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 28 shows the X-ray powder diffraction pattern of the bromide salt (Form K) of compound (I) as obtained by Example 11. The diffraction pattern was obtained by irradiation of the crystalline product using Bruker AXS D8 Advance.
  • Figure 29 shows a DSC thermogram (lower trace) of the HBr salt Form K of compound (I) as obtained by Example 11 , using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 74 and 95°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851e at a heating rate of 10°C.min "1 .
  • Figure 30 shows a DSC thermogram (lower trace) of the mesylate salt Form L of compound (I) as obtained by Example 12, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 132°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA SDTA 851e at a heating rate of 10°C.min "1 .
  • Figure 31 shows a DSC thermogram (lower trace) of the maleate salt Form M of compound (I) as obtained by Example 13, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 123°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA SDTA 851e at a heating rate of 10°C.min "1 .
  • Figure 32 shows a DSC thermogram (lower trace) of the gentisate salt Form O of compound (I) as obtained by Example 15, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 99°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA SDTA 851 e at a heating rate of 10°C.min "1 .
  • Figure 33 shows a DSC thermogram (lower trace) of the fumarate salt Form P of compound (I) as obtained by Example 16, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 143°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA SDTA 851 e at a heating rate of 10°C.min "1 .
  • Figure 34 shows a DSC thermogram (lower trace) of the L-malate salt Form Q of compound (I) as obtained by Example 17, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 92°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851 e at a heating rate of 10°C.min "1 .
  • Figure 35 shows a DSC thermogram (lower trace) of the L-malate salt Form R of compound (I) as obtained by Example 18, using ettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 114°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851 e at a heating rate of 10°C.min "1 .
  • Figure 36 shows a DSC thermogram (lower trace) of the HCI salt Form H of compound (I) as obtained by Example 8, using Mettler DSC823e at a heating rate of 10°C.min ⁇ 1 (peak max observed at 68, 87, 104 and 148°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851e at a heating rate of 10°C.min ⁇ 1 .
  • Figure 37 shows a DSC thermogram (lower trace) of the HCI salt Form I of compound (I) as obtained by Example 9, using Mettler DSC823e at a heating rate of 10°C.min '1 (peak max observed at 120 and 139°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA/SDTA 851e at a heating rate of 10°C.min ⁇ 1 .
  • Figure 38 shows a DSC thermogram (lower trace) of the HBr salt Form J of compound (I) as obtained by Example 10, using Mettler DSC823e at a heating rate of 10°C.min "1 (peak max observed at 142°C).
  • the upper trace shows TGA analysis for the same salt using a Mettler TGA SDTA 851 e at a heating rate of 10°C.min ⁇
  • XRPD patterns referred to herein are obtained using copper K-alpha radiation.
  • XRPD values as described in the accompanying specification, figures or tables refer to approximate values. Where the reference is to XRPD values listed in the tables, this refers to the 2-theta values, independent of any other parameters listed in the tables, such as peak intensity or the like.
  • XRPD on the phosphate (Forms B, C), citrate (Form F), benzenesulfonic acid (Form G) and L-tartrate (Form D) salts were carried out using a Bruker AXS C2 GADDS diffractometer as described below.
  • XRPD on the hydrochloride (Forms H, I), hydrobromide (Forms J, K), mesylate (Form L), maleate (Form M), gentisate (Form O), fumarate (Form P), and L-malate (Forms, Q, R) salts were carried out using a Bruker AXS D8 Advance diffractometer as described below.
  • XRPD on free base (Form A) compound (I) and the L-tartrate salt (Form E) was carried out using PANalytical diffractometer as described below.
  • X-Ray Powder Diffraction patterns were collected on a Bruker AXS C2 GADDS diffractometer using Cu Ka radiation (40 kV, 40 mA), automated XYZ stage, laser video microscope for auto-sample positioning and a HiStar 2-dimensional area detector.
  • X-ray optics consists of a single Gobel multilayer mirror coupled with a pinhole collimator of 0.3 mm. The beam divergence, i.e. the effective size of the X-ray beam on the sample, was approximately 4 mm. A ⁇ - ⁇ continuous scan mode was employed with a sample detector distance of 20 cm which gives an effective 2 ⁇ range of 3.2°-29.7°. Typically the sample would be exposed to the X-ray beam for 120 seconds.
  • the software used for data collection was GADDS for WNT 4.1.16 and the data were analysed and presented using Diffrac Plus EVA v 9.0.0.2 or v 13.0.0.2.
  • X-Ray Powder Diffraction patterns were collected on a Bruker D8 diffractometer using Cu Ka radiation (40kV, 40mA), ⁇ -2 ⁇ goniometer, and divergence of V4 and receiving slits, a Ge monochromator and a Lynxeye detector.
  • the instrument is performance checked using a certified Corundum standard (NIST 1976).
  • the software used for data collection was Diffrac Plus XRD Commander v2.5.0 and the data were analysed and presented using Diffrac Plus EVA v 11.0.0.2 or v 13.0.0.2. Unless otherwise stated, XRPD patterns collected on this instrument were used to produce the XRPD peak lists.
  • Step size 0.05 °2 ⁇
  • Samples run under non-ambient conditions were mounted on a silicon wafer with heat conducting compound. The sample was then heated to the appropriate temperature at ca. 10 "C.rnin "1 and subsequently held isothermally for ca 1 minute before data collection was initiated.
  • X-Ray Powder Diffraction patterns were collected on a PANalytical diffractometer using Cu Ka radiation (45kV, 40mA), goniometer, focusing mirror, divergence slit (1/2"), soller slits at both incident and divergent beam (4mm) and a PIXcel detector.
  • the software used for data collection was X'Pert Data Collector, version 2.2f and the data was presented using X'Pert Data Viewer, version 1.2d.
  • DSC data were collected on a Mettler DSC 823e equipped with a 50 position autosampler.
  • the instrument was calibrated for energy and temperature using certified indium. Typically 0.5-3 mg of each sample, in a pin-holed aluminium pan, was heated at 10°C.min "1 from 25°C to 350°C. A nitrogen purge at 50 ml.min "1 was maintained over the sample.
  • the instrument control and data analysis software was STARe v9.10.
  • DSC data was collected on a PerkinElmer Pyris 6 DSC or DSC 4000. The instrument was verified for energy and temperature calibration using certified indium. A predefined amount of sample (in mg) was placed in a pin holed aluminium pan and heated at 20°C.min "1 from 30°C to 320°C. The instrument control and data analysis was Pyris Software v9.0.1.0174.
  • TGA data were collected on a Mettler TGA/SDTA 851 e equipped with a 34 position autosampler.
  • the instrument was temperature calibrated using certified indium. Typically 5-30 mg of each sample was loaded onto a pre-weighed aluminium crucible and was heated at 10°C.min "1 from ambient temperature to 350°C. A nitrogen purge at 50ml.min "1 was maintained over the sample.
  • the instrument control and data analysis software was STARe V9.10.
  • TGA data was collected on a Pyris 1 TGA equipped with a 20 position autosampler.
  • the instrument was calibrated using certified indium. 6.329 mg of the sample was loaded onto a pre-weighed aluminium crucible and was heated at 20 °C.min "1 (or 40 °C.min "1 ) from ambient temperature to 500 °C. A nitrogen purge at 20 ml.min "1 was maintained over the sample.
  • the instrument control and data analysis was Pyris Software v9.0 1.0174. Polarised Light Microscopy (PLM)
  • Samples were studied on a Leica LM/DM polarised light microscope with a digital videocamera for image capture. A small amount of each sample was placed on a glass slide, mounted in immersion oil and covered with a glass slip, the individual particles being separated as well as possible. The sample was viewed with appropriate magnification and partially polarised light, coupled to a ⁇ false-colour filter.
  • Samples were studied on a Leica DME polarised light microscope with a digital video camera for image capture. A small amount of the sample was placed on a glass slide and covered with a glass slip, individual particles being separated as well as possible. The sample was viewed with appropriate magnification (10x 0.22) and fully polarised light to assess crystallinity.
  • Hot Stage Microscopy was carried out using a Leica LM/DM polarised light microscope combined with a Mettler-Toledo MTFP82HT hot-stage and a digital video camera for image capture. A small amount of each sample was placed onto a glass slide with individual particles separated as well as possible. The sample was viewed with appropriate magnification and partially polarised light, coupled to a ⁇ false-colour filter, whilst being heated from ambient temperature typically at 10-20°C.min "1 .
  • Sorption isotherms were obtained using a SMS DVS Intrinsic moisture sorption analyser, controlled by SMS Analysis Suite software.
  • the sample temperature was maintained at 25 °C by the instrument controls.
  • the humidity was controlled by mixing streams of dry and wet nitrogen, with a total flow rate of 200 ml.min "1 .
  • the relative humidity was measured by a calibrated Rotronic probe (dynamic range of 1.0-100 %RH), located near the sample.
  • the weight change, (mass relaxation) of the sample as a function of %RH was constantly monitored by the microbalance (accuracy ⁇ 0.005 mg). Typically 5-20 mg of sample was placed in a tared mesh stainless steel basket under ambient conditions.
  • the sample was loaded and unloaded at 40%RH and 25°C (typical room conditions).
  • a moisture sorption isotherm was performed as outlined below (2 scans giving 1 complete cycle).
  • the standard isotherm was performed at 25°C at 10 %RH intervals over a 0.5-90 %RH range.
  • Sorption isotherms were obtained using a Hiden Isochema Moisture Sorption Analyser (IGAsorp) controlled by IGAsorp Systems Software V6.50.48.
  • the sample temperature was maintained at 25 °C by the instrument controls.
  • the humidity was controlled by mixing streams of dry and wet nitrogen, with a total flow rate of 250ml. min "1 .
  • the instrument was verified for relative humidity content by measuring three calibrated Rotronic salt solutions (10-50-88 %).
  • the weight change of the sample as a function of %RH was monitored by microbalance (accuracy ⁇ 0.005 mg).
  • a defined amount of sample was placed in a tared mesh stainless steel basket under ambient conditions.
  • a full experimental cycle consisted of two scans (sorption and desorption) at a constant temperature (25°C) and 10% RH intervals over a 10-90% RH range (90 minutes for each humidity level).
  • Thermodynamic Aqueous Solubility was determined by suspending sufficient compound in HPLC grage water to give a maximum final concentration of ⁇ 10 mg.ml " of the parent free-form of the compound. The suspension was equilibrated at 25°C for 24 hours then the pH was measured.
  • the suspension was then filtered through a glass fibre C filter into a 96 well plate.
  • the filtrate was then diluted by a factor of 101.
  • Quantitation was by HPLC with reference to a standard solution of approximately 0.1 mg.ml "1 in DMSO. Different volumes of the standard, diluted and undiluted sample solutions were injected. The solubility was calculated using the peak areas determined by integration of the peak found at the same retention time as the principal peak in the standard injection.
  • Compound (I) may be prepared in accordance with the methodology described in WO 2008/122767 (Cyclacel Limited).
  • Compound (I) may be prepared via the following procedure: A solution of (4,6-dimethylpyridin-3ylmethyl)-(2-fluoro-9-isopropyl 9H-purin-6-yl)-amine (30g), (2R,3S)-3-amino-pentan-2-ol (29.5g) and DIEA (33.0mL) in ethylene glycol (270mL) was heated at 125°C under nitrogen overnight. A further 0.5 equivalents of (2R,3S)-3-amino-pentan-2-ol (4.9g) was added and the reaction stirred for an additional 6 hours.
  • Compound (I) was crystallised from TBE by the following method. MTBE (2 vol) was added to compound (I) and heated to reflux. The mixture was held at reflux for 30-60 minutes before the temperature was reduced to 50°C (held for 2 hours). The suspension was allowed to cool slowly to room temperature before being filtered and rinsed with MTBE (3 x 1 vol). The solids were dried in vacuum oven at 40 °C for 8 hours to afford the desired crystalline free base (mass recovery 84.5%, LC purity 97.4 %).
  • Aqueous solubility was determined by suspending sufficient compound in HPLC grade water to give a maximum final concentration of ⁇ 10mg.ml "1 of the parent free-form of the compound. The suspension was equilibrated at 25°C for 24 hours. The suspension was then filtered through a filter into an HPLC vial. The filtrate was then diluted by an appropriate factor. Quantification was executed by HPLC with reference to a standard solution of 0.5mg in 1mL acetonitrile / water (1 :1 ). Different volumes of the standard, diluted and undiluted sample solutions were injected. The solubility was calculated using the peak areas determined by integration of the peak found at the same retention time as the principal peak in the standard injection. The aqueous solubility was determined to be 0.329mg/mL. Analysis of Form A post solubility study showed no change by XRPD ( Figure 18).
  • Example 2 Preparation of Citrate Salt (Form F) of Compound (I)
  • Compound (I) (100mg, 0.25mmol, 1 equiv), citric acid (49mg, 0.26mmol, 1.02 equiv) and ethyl acetate (1 ml, 10vol) were charged to a vial and stirred under ambient conditions for 24 hours - a small lump of sticky solid remained undissolved.
  • the mixture was stored in a shaker on a heat/cool cycle (60°C/RT, 4 h) for 68 h.
  • the resultant white precipitate was isolated by vacuum filtration, washed with EtOAc (2 x 500 ⁇ , 2 x 5 vol) and dried in a vacuum oven at 30°C for 16 hours to yield the citrate salt as a white solid (53mg, 40 % yield).
  • the 1 H NMR spectrum of the citrate salt was consistent with structure and a set of diastereotopic peaks was present corresponding to the citrate anion.
  • 1 H NMR analysis also confirmed the presence of residual ethyl acetate.
  • XRPD analysis confirmed the material to be crystalline.
  • DSC analysis showed two endothermic events: a sharp peak, corresponding to the melt, with an onset of 145°C and a broad event with an onset of 165°C.
  • TGA analysis showed no weight loss before or during the melt, followed by decomposition above 180°C, confirming the second endothermic event in the DSC is likely to be decomposition.
  • TGA analysis also proved the material is not a solvate.
  • a sample of the product was stored in a humidity chamber at 25°C and 94% RH for 3 days, after which time the material was slightly tacky, though it had not deliquesced.
  • XRPD analysis of this material showed the same pattern as obtained for the initial product, but with a significant amorphous halo.
  • a second sample was stored in a humidity chamber at 25°C and 75% RH for 70 hours, after which time the sample appeared unchanged and the XRPD pattern obtained for this material was consistent with that of the original product.
  • GVS analysis conformed that no hydrate is formed at high RH, though the material proved to be hygroscopic above 70% RH.
  • the resultant white precipitate was isolated by vacuum filtration, washed with TBME (3 x 500 ⁇ , 3 x 5 vol) and dried in a vacuum oven at 30°C for 16 hours to yield the benzenesulfonic acid salt as a white solid (65mg, 47% yield).
  • TGA analysis exhibited a weight loss of 1.1 % between 75 and 120°C that was not accompanied by an endotherm in the DSC and is attributed to the loss of unbound solvent, proving the material to be non-solvated.
  • Deliquescence of a sample of the product was observed after storage in a humidity chamber at 25°C and 94% RH for 2 hours.
  • a second sample was stored in a humidity chamber at 25°C and 75% RH for 70 hours, after which time the sample was slightly tacky.
  • the XRPD pattern obtained for this material was consistent with that of the original product, but with a slightly larger amorphous halo.
  • the 1 H NMR spectrum of the tartrate salt was consistent with structure and exhibited a singlet at 4.31 ppm corresponding to the tartrate anion.
  • XRPD analysis confirmed the material to be crystalline.
  • DSC analysis showed a single endothermic event with an onset of 147°C that was confirmed, by hot stage microscopy, to be a melt.
  • TGA analysis showed no weight loss before or during the melt, followed by decomposition above 200°C, showing that this material is not a solvate.
  • a sample of product was stored in a humidity chamber at 25°C and 94% RH for 70 hours, after which time the material was slightly tacky, though it had not deliquesced.
  • XRPD analysis of this material showed the presence of some peaks corresponding to those in the pattern acquired for the original product, though a significant amorphous halo was also visible, due to the uptake of water.
  • a second sample was stored in a humidity chamber at 25°C and 75% RH for 4 days, after which time the sample was unchanged.
  • the XRPD pattern obtained for this material was consistent with that of the original product.
  • GVS analysis confirmed that no hydrate is formed at high RH, though the material proved to be hygroscopic above 70% RH.
  • Form E of the L-Tartrate salt of compound (I) was also prepared by slurry conversion from four different solvents (ethyl acetate, IPA, IMS or acetonitrile).
  • a 1 :1 mixture of Form by weight of D Form E L-Tartrate salt (200 mg total) was heated at 45°C over 48 hours in 2ml of solvent prior to filtration and analysis.
  • Form E was produced in each slurry (purity ⁇ 98 %).
  • CYC065 free base Form A (0.2g) was dissolved in ethanol (9 vol, 1.8mL) and heated at reflux. A solution of tartaric acid (1 eq, 0.076g) in water (1.7 vol, 0.34mL) / ethanol (1 vol, 0.2mL) was added dropwise maintaining the temperature at reflux. The resulting solution was then polish filtered before cooling to 70°C. A seed of Form E was added giving a cloudy solution. The batch was stirred at 70°C for 1 hour before cooling to room temperature. After stirring at room temperature for 2 hours, the solid was filtered, washed with ethanol (2 x 0.5ml_) and pulled dry.
  • the XRPD pattern obtained for the product was similar, though not identical to, the corresponding material crystallised from IPA (see Example 7). These results suggest that crystallisation from ethanol yields a different polymorph of the resultant phosphate salt than crystallisation from IPA. DSC analysis showed two broad endothermic events with onsets of 67 and 125°C. The first endotherm was comparable with the first event observed in the DSC traces of the material formed in IPA (see Example 7). Interestingly, the second endotherm had a significantly higher onset (123°C) than the comparable material obtained from IPA (116°C), again suggesting the presence of a different solid form.
  • TGA analysis showed a weight loss of 2.9%, between 45 and 98°C, corresponding to the first endotherm in the DSC, thus confirming that the first endotherm observed in the DSC was due to the loss of bound solvent. At this stage, it was not confirmed whether this solvent loss was due to the loss of IPA or water, or a mixture of both. TGA analysis showed no weight loss associated with the second event observed in the DSC, followed by decomposition above 220°C. Hot stage microscopy confirmed the second endotherm observed in the DSC to be a melt.
  • Variable temperature XRPD analysis was undertaken on a sample of Form C in order to elucidate if the loss of solvent observed in the DSC resulted in a change of form.
  • the sample was heated to each temperature, held for 3 minutes to allow equilibration and an XRPD pattern was collected.
  • the material was taken to 100°C, in 10 degree increments, a pattern was collected, the sample was held at 100°C for 15 minutes and a second pattern was collected.
  • the sample was cooled back to RT and a final reference pattern was obtained.
  • the resultant white precipitate was isolated by vacuum filtration and washed with IPA (2 x 1.5 ml, 2 x 3 vol) and dried under suction. Two distinct types of material were clearly visible in the cake - a dry white powdery solid round the outside and a sticky off white solid in the centre. The dry solid was isolated to yield the phosphate salt as a white solid (110mg, 15 % yield).
  • the 1 H NMR spectrum of the product was consistent with structure, a minor amount of residual IPA was also noted.
  • the XRPD confirmed that the product was in crystalline form.
  • the DSC trace exhibited two events with onsets of 67 and 116°C and the TGA exhibited a weight loss of 2.6%, between 45 and 98°C, corresponding to the loss of bound solvent during the first endothermic event in the DSC. At this stage it was not confirmed whether this solvent loss was due to loss of IPA or water, or a mixture of both.
  • the TGA showed no weight loss associated with the second event in the DSC, followed by decomposition above 220°C. Hot stage microscopy confirmed the second endotherm observed in the DSC to be a melt.
  • Variable temperature XRPD analysis was undertaken on the product in order to elucidate if the loss of solvent observed in the DSC resulted in a change of form.
  • the sample was heated to each temperature, held for 3 minutes to allow for equilibration and an XRPD pattern was collected.
  • the material was taken to 100°C, in 10 degree increments, a pattern was collected then the sample was held at 100°C for 15 minutes and a second pattern was collected.
  • the sample was cooled back to RT and a final reference pattern was obtained.
  • the second heat showed no endothermic event corresponding to the loss of solvent therefore showing that this process is irreversible under an inert atmosphere of nitrogen.
  • a series of TGA experiments were undertaken to clarify how quickly the material rehydrates under ambient conditions. A series of samples were taken to 100°C then cooled to 25°C under nitrogen using the TGA equipment. The samples were stored under ambient conditions (RT in air) for varying times and then the TGA experiment was re-run. As a comparison a heat/cool/heat experiment was undertaken under an inert atmosphere of nitrogen using the TGA; a sample was heated to 100°C, cooled to 25°C and heated to 100°C for a second time.
  • a sample of product was stored in a humidity chamber at 25°C and 94% RH for 88 hours, after which time no deliquescence was observed.
  • the XRPD pattern obtained for this material matched those acquired for the phosphate salt crystallised from ethanol (see Example 6), rather than that of the parent compound.
  • the DSC analysis exhibited two discreet melts, corresponding to the crystalline form produced by crystallisation from IPA and that produced from ethanol, with the melt of the ethanol form appearing to be the dominant event.
  • GVS analysis was undertaken at 25°C and showed the material not to be hygroscopic as a gradual uptake of only -1.5 weight % of water was observed above 80% RH.
  • the mixture had concentrated to approximately 1/3 original volume during the maturation.
  • the resultant solid was isolated by vacuum filtration and washed with TBME (2 x 5ml). The solid was dried under suction and in a vacuum oven at 30 ° C / 3mbar for 20h to yield the hydrochloride salt as a white solid (158.69mg, 42% based on mono-chloride salt formation).
  • VT-XRPD analysis of the product suggested conversion of HCI Pattern 1 (Form H) to a new pattern (HCI Pattern 4) above 80 ° C followed by complete loss of crystallinity above 100 ° C.
  • Visual analysis of the sample used for VT-XRPD showed the formation of a foam at elevated temperatures, once crystallinity had been lost, indicative of a loss of volatile material (possibly TBME or excess HCI).
  • TGA shows a weight loss of 3.4% from 45 to 105 ° C, equivalent to 0.8 equiv H 2 0 and greater than the observed levels of TBME. The weight loss could indicate the presence of a solvate that desolvates to the different form observed by VT-XRPD.
  • HCI Pattern 2 (Form I) material was a mono-chloride salt that appears to be isostructural with HBr Pattern 1.
  • HSM shows a melt corresponding to the broad endotherms observed in the DSC, whilst VT-XRPD shows no change in form before the melt.
  • HCI Pattern 2 (Form I) showed conversion to HCI Pattern 1 (Form H) upon storage at 40 ° C / 75%. This result may indicate that HCI Pattern 1 (Form H) is likely to be a mono- chloride salt.
  • Proton NMR and TGA analyses were undertaken on this sample in an attempt to clarify the properties of HCI Pattern 1 (Form H) material, as the analysis sample from Example 8 was complicated by the presence of residual TBME and possibly excess HCI.
  • Proton NMR confirmed the absence of residual TBME, whilst TGA showed a stepped weight loss of 4.6%, equivalent to 1.2 equiv of water.
  • HBr 48 wt % solution in water (77 ⁇ , 0.45mmol, 0.9 equiv) was added dropwise to a solution of free base of compound (I) (200.46mg, 0.50mmol, 1 equiv) in EtOAc (10ml, 50 relative volumes) at RT with swirling - a sticky white solid formed instantaneously.
  • EtOAc 10ml, 50 relative volumes
  • the sample was stored in a shaker on a heat / cool cycle (40°C / RT, 4h at each) for 18h.
  • the resultant sticky solid was isolated by vacuum filtration and washed with EtOAc (2 x 2ml).
  • the solid was dried under suction and in a vacuum oven at 30°C / 3mbar for 14h to yield the hydrobromide salt as a yellow solid (86.54mg, 40% based on mono-bromide salt formation).
  • HBr Pattern 1 (Form J) to be a partially crystalline mono-bromide salt that appears to be isostructural with HCI Pattern 2 (Form I).
  • HSM and DSC analyses suggest a melt with an onset of approximately 138 ° C.
  • HCI Pattern 2 (Form I)
  • Storage at 40 ° C / 75% RH showed conversion to a new Pattern - HBr Pattern 2 (Form K).
  • HBr Pattern 1 (Form J) at 40 ° C / 75% relative humidity.
  • HBr Pattern 1 (Form J) showed deliquescence after 15h, but crystallisation was observed upon extended storage of 7 days.
  • Methanesulfonic acid (59 ⁇ , 0.91 mmol, 0.9 equiv) was added dropwise to a stirring solution of free base compound (I) (400.08mg, 1.0 mmol, 1 equiv) in TBME (20ml, 50 relative volumes) at RT - a sticky white solid formed instantaneously - and the mixture was stirred at RT for 16h. A precipitate appeared to have formed and an aliquot was taken and isolated by vacuum filtration. A sticky solid was obtained from the isolated sample that did not improve with drying. The remaining sample was stirred at RT for a further 8h, heated to 40 ° C and stirred for a further 1.5h, then cooled to RT and stirred for 14h.
  • Mesylate Pattern 1 was a non-solvated mono mesylate salt with a melt at approximately 126 ' C.
  • the aqueous solubility was determined to be ⁇ 140mg.ml '1 , the highest of the salts obtained during the course of this work.
  • the sample was found to be hygroscopic as deliquescence was observed inside 15 h at 40°C and 75% RH.
  • Free base compound (I) 400.85mg, 1.01mmol, 1 equiv
  • maleic acid 117.01 mg, 1.01mmol, 1 equiv
  • TBME 20ml, 50 relative volumes
  • Free base compound (I) 400.27 mg, 1.01 mmol, 1 equiv
  • gentisic acid 155.25 mg, 1.01 mmol, 1 equiv
  • EtOAc 8 ml, 20 relative volumes
  • the mixture was stored in a shaker on a heat / cool cycle (40 ° C / RT, 4 h at each) for 63 h to give a light yellow solution.
  • the mixture was cooled to 5 °C for 24 h - no precipitation was observed.
  • the mixture was cooled to -18 "C for 24 h - a light yellow solid was formed.
  • the solid was isolated by vacuum filtration using glassware pre- cooled to -18 ° C.
  • Gentisate Pattern 2 (Form O) material to be a mono Gentisate acid salt containing approximately 0.5 equiv of acetonitrile that is lost in conjunction with an endothermic event. Further analyses to elucidate if the sample is a hemi-solvate or contains trapped solvent were not possible due to the minor amount of material produced.
  • Free base compound (I) 400.18mg, 1.01 mmol, 1 equiv
  • fumaric acid 116.71 mg, 1.01 mmol, 1 equiv
  • EtOAc 4ml, 10 relative volumes
  • the solid was isolated by vacuum filtration, washed with EtOAc (3 x 2ml), dried under suction and in a vacuum oven at 30°C / 3mbar for 15h to yield the fumarate salt as a yellow solid (261.35mg, 50% yield based on mono- fumarate salt formation).
  • Free base compound (I) 400.19mg, 1.01mmol, 1 equiv
  • L-malic acid (135.35mg, 1.01mmol, 1 equiv)
  • EtOAc 20ml, 50 relative volumes
  • the solid was isolated by vacuum filtration, washed with EtOAc (2 x 3ml), dried under suction and in a vacuum oven at 30 ° C / 3mbar for 14h to yield the L-malate salt as a white solid (325.99mg, 61% yield based on mono- L-malate salt formation).
  • L-malate Pattern 1 material was a non-solvated mono malate salt with a melt at approximately 81 ° C.
  • L-malate Pattern 1 material appeared to be hygroscopic, as deliquescence occurred within 15h at 40 ° C / 75% RH. However, upon extended storage at 40°C / 75% RH (72h) crystallisation of a new solid form was observed.
  • XRPD analysis confirmed this material to be inconsistent with L-malate Pattern 1 (Form Q) and was given the identification of L-malate Pattern 2 (Form R).
  • L-malate Form Q 75.45mg was stored at 40°C / 75% RH for 72h - deliquescence was observed inside 2h and crystallisation had occurred inside 72h.
  • the sample was dried in a vacuum oven at 40 ° C / 3mbar for 18h to yield the L-malate (Form R) as a white solid.
  • NMR analysis of the sample of Form R formed during the storage of Form Q at 40 ° C / 75% RH confirmed it to be a mono-malate salt.
  • DSC analysis appeared to suggest the material to be non-solvated with a higher melting point (103.5"C) than L-malate Form Q.

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ES2613716T3 (es) 2017-05-25
KR101860806B1 (ko) 2018-05-24
JP6114849B2 (ja) 2017-04-12
JP2016128501A (ja) 2016-07-14
ES2694289T3 (es) 2018-12-19
US20150148354A1 (en) 2015-05-28
EP2526101A1 (en) 2012-11-28
EP3150602A1 (en) 2017-04-05
CN102985423B (zh) 2017-08-08
TR201816159T4 (tr) 2018-11-21
GB201001075D0 (en) 2010-03-10
US20130072504A1 (en) 2013-03-21
JP5951506B2 (ja) 2016-07-13
KR101927083B1 (ko) 2018-12-10
SG182439A1 (en) 2012-08-30
EP2526101B1 (en) 2016-12-07
PL2526101T3 (pl) 2017-08-31
JP2013518041A (ja) 2013-05-20
US8889861B2 (en) 2014-11-18
KR20120124450A (ko) 2012-11-13
CN102985423A (zh) 2013-03-20
EP3150602B1 (en) 2018-08-01
CN107400134B (zh) 2020-09-29

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